Amide-Linked C4″-saccharide modification of krn7000 provides potent stimulation of human invariant NKT cells and anti-tumor immunity in a humanized mouse model
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Saavedra Ávila, Noemí Alejandra
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Amide-Linked C4″-saccharide modification of krn7000 provides potent stimulation of human invariant NKT cells and anti-tumor immunity in a humanized mouse model
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Abstract
Activation of invariant natural killer T (iNKT) cells
by α-galactosylceramides (α-GalCers) stimulates strong immune
responses and potent anti-tumor immunity. Numerous modifications
of the glycolipid structure have been assessed to derive
activating ligands for these T cells with altered and potentially
advantageous properties in the induction of immune responses.
Here, we synthesized variants of the prototypical α-GalCer,
KRN7000, with amide-linked phenyl alkane substitutions on the
C4″-position of the galactose ring. We show that these variants
have weak iNKT cell stimulating activity in mouse models but
substantially greater activity for human iNKT cells. The most
active of the C4″-amides in our study showed strong anti-tumor
effects in a partially humanized mouse model for iNKT cell responses. In silico analysis suggested that the tether length and degree of
flexibility of the amide substituent affected the recognition by iNKT cell antigen receptors of the C4″-amide substituted glycolipids
in complex with their antigen presenting molecule CD1d. Our findings establish the use of stable C4″-amide linked additions to the
sugar moiety for further exploration of the immunological effects of structural modifications of iNKT cell activating glycolipids and
highlight the critical need for more accurate animal models to assess these compounds for immunotherapeutic potential in humans.
Patrocinador
National Institutes of Health (NIH) - USA R01 GM111849
Aparece en contenido como:NIH
R01 AI045889
Aparece en contenido como:NIH
National Science Foundation (NSF) DGE-1247393
NIH/NCI Cancer Center Service Grant P30 CA13330
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ACS Chem. Biol. 2020, 15, 3176−3186
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